Discovery of IHMT-MST1-58 as a Novel, Potent, and Selective MST1 Inhibitor for the Treatment of Type 1/2 Diabetes.
Yun WuZiping QiBeilei WangJunjie WangQingwang LiuAoli WangChenliang ShiBin ZhouQianmao LiangWenliang WangFengming ZouShuang QiZuowei WangLi WangWenchao WangJing LiuQing-Song LiuPublished in: Journal of medicinal chemistry (2022)
The critical pathogenesis of type 1 diabetes (T1D)/type 2 diabetes (T2D) is the physical status, mass, and function of pancreatic β cells. Mammalian STE20-like protein 1 kinase (MST1) plays vital roles in the apoptosis and insulin secretion of β cells. Here, we discovered a novel, potent, and selective MST1 inhibitor 19 (IC 50 = 23 nM), which inhibited the phosphorylation of MST1-protected β cells from the damage of inflammatory cytokines in vitro. In vivo, it displayed acceptable pharmacokinetic properties in different species. In the STZ-induced T1D/T2D mouse models, both monotherapy of 19 and in combination with metformin led to the decline of fasting blood glucose and showed protective effect of β cells. In addition, the combination of 19 and metformin decreased the hemoglobin A1c level. Together, our study suggested that 19 might be a useful pharmacological tool to study MST1-mediated physiology and pathology as well as a potential drug candidate for diabetes.
Keyphrases
- cell cycle arrest
- induced apoptosis
- blood glucose
- type diabetes
- glycemic control
- endoplasmic reticulum stress
- oxidative stress
- cell death
- cardiovascular disease
- protein kinase
- signaling pathway
- insulin resistance
- diabetic rats
- clinical trial
- physical activity
- emergency department
- mental health
- skeletal muscle
- mouse model
- combination therapy
- drug induced
- climate change
- weight loss
- human health